Whole abdominopelvic intensity-modulated radiation therapy for desmoplastic small round cell tumor after surgery

Chelsea C. Pinnix; Hiral P. Fontanilla; Andrea Hayes-Jordan; Vivek Subbiah; Stephen D. Bilton; Eric L. Chang; David R. Grosshans; Mary F. McAleer; Eric P. Sulman; Shiao Y. Woo; Peter Anderson; Holly L. Green; Anita Mahajan

doi:10.1016/j.ijrobp.2011.06.1985

Whole abdominopelvic intensity-modulated radiation therapy for desmoplastic small round cell tumor after surgery

Chelsea C. Pinnix, Hiral P. Fontanilla, Andrea Hayes-Jordan, Vivek Subbiah, Stephen D. Bilton, Eric L. Chang, David R. Grosshans, Mary F. McAleer, Eric P. Sulman, Shiao Y. Woo, Peter Anderson, Holly L. Green, Anita Mahajan

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Abstract

Purpose: Desmoplastic small round cell tumor (DSCRT) is an uncommon pediatric tumor with a poor prognosis. Aggressive multimodality therapy is the current treatment approach; however. treatment toxicity is of concern. We report our results with whole abdominopelvic intensity-modulated radiation therapy (WAP-IMRT) as a component of multimodality therapy for DSCRT at a single institution. Materials/Methods: Medical records of all patients with DSCRT who received WAP-IMRT as part of definitive treatment at MD Anderson (2006-2010) were identified and reviewed. Results: Eight patients with DSRCT received WAP-IMRT with a median follow-up of 15.2 months. All patients received multiple courses of chemotherapy followed by surgical debulking of intra-abdominal disease; seven also had intraoperative hyperthermic cisplatin. WAP-IMRT was delivered to a total dose of 30 Gy postoperatively; four patients received a simultaneous boost (6-10 Gy) to sites of gross residual disease. Seven patients received concurrent chemotherapy during WAP-IMRT. No Radiation Therapy Oncology Group Grade 4 nausea, vomiting, or diarrhea occurred during RT. Red-cell transfusions were given to two patients to maintain hemoglobin levels >10 g/dL. Grade 4 cytopenia requiring growth factor support occurred in only one patient; no other significant cytopenias were noted. WAP-IMRT resulted in 25% lower radiation doses to the lumbosacral vertebral bodies and pelvic bones than conventional RT plans. The median time to local or distant failure after WAP-IMRT was 8.73 months in seven patients. One patient who had completed RT 20 months before the last follow-up remains alive without evidence of disease. Five patients (63%) experienced treatment failure in the abdomen. Distant failure occurred in three patients (37.5%). Conclusions: WAP-IMRT with concurrent radiosensitizing chemotherapy was well tolerated after aggressive surgery for DSCRT. Enhanced bone sparing with IMRT probably accounts for the low hematologic toxicity (vs. conventional WAP-RT). This modality should be considered as an additional local-regional control option for DSRCT.

Original language	English (US)
Pages (from-to)	317-326
Number of pages	10
Journal	International Journal of Radiation Oncology Biology Physics
Volume	83
Issue number	1
DOIs	https://doi.org/10.1016/j.ijrobp.2011.06.1985
State	Published - May 1 2012

Keywords

Desmoplastic small round-cell tumor (DSRCT)
IMRT
Pediatric cancer
Peritoneal sarcomatosis
Sarcoma
Whole abdominopelvic radiotherapy

ASJC Scopus subject areas

Radiation
Oncology
Radiology Nuclear Medicine and imaging
Cancer Research

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10.1016/j.ijrobp.2011.06.1985

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Pinnix, C. C., Fontanilla, H. P., Hayes-Jordan, A., Subbiah, V., Bilton, S. D., Chang, E. L., Grosshans, D. R., McAleer, M. F., Sulman, E. P., Woo, S. Y., Anderson, P., Green, H. L., & Mahajan, A. (2012). Whole abdominopelvic intensity-modulated radiation therapy for desmoplastic small round cell tumor after surgery. International Journal of Radiation Oncology Biology Physics, 83(1), 317-326. https://doi.org/10.1016/j.ijrobp.2011.06.1985

Pinnix, CC, Fontanilla, HP, Hayes-Jordan, A, Subbiah, V, Bilton, SD, Chang, EL, Grosshans, DR , McAleer, MF, Sulman, EP, Woo, SY, Anderson, P, Green, HL & Mahajan, A 2012, 'Whole abdominopelvic intensity-modulated radiation therapy for desmoplastic small round cell tumor after surgery', International Journal of Radiation Oncology Biology Physics, vol. 83, no. 1, pp. 317-326. https://doi.org/10.1016/j.ijrobp.2011.06.1985

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abstract = "Purpose: Desmoplastic small round cell tumor (DSCRT) is an uncommon pediatric tumor with a poor prognosis. Aggressive multimodality therapy is the current treatment approach; however. treatment toxicity is of concern. We report our results with whole abdominopelvic intensity-modulated radiation therapy (WAP-IMRT) as a component of multimodality therapy for DSCRT at a single institution. Materials/Methods: Medical records of all patients with DSCRT who received WAP-IMRT as part of definitive treatment at MD Anderson (2006-2010) were identified and reviewed. Results: Eight patients with DSRCT received WAP-IMRT with a median follow-up of 15.2 months. All patients received multiple courses of chemotherapy followed by surgical debulking of intra-abdominal disease; seven also had intraoperative hyperthermic cisplatin. WAP-IMRT was delivered to a total dose of 30 Gy postoperatively; four patients received a simultaneous boost (6-10 Gy) to sites of gross residual disease. Seven patients received concurrent chemotherapy during WAP-IMRT. No Radiation Therapy Oncology Group Grade 4 nausea, vomiting, or diarrhea occurred during RT. Red-cell transfusions were given to two patients to maintain hemoglobin levels >10 g/dL. Grade 4 cytopenia requiring growth factor support occurred in only one patient; no other significant cytopenias were noted. WAP-IMRT resulted in 25% lower radiation doses to the lumbosacral vertebral bodies and pelvic bones than conventional RT plans. The median time to local or distant failure after WAP-IMRT was 8.73 months in seven patients. One patient who had completed RT 20 months before the last follow-up remains alive without evidence of disease. Five patients (63%) experienced treatment failure in the abdomen. Distant failure occurred in three patients (37.5%). Conclusions: WAP-IMRT with concurrent radiosensitizing chemotherapy was well tolerated after aggressive surgery for DSCRT. Enhanced bone sparing with IMRT probably accounts for the low hematologic toxicity (vs. conventional WAP-RT). This modality should be considered as an additional local-regional control option for DSRCT.",

keywords = "Desmoplastic small round-cell tumor (DSRCT), IMRT, Pediatric cancer, Peritoneal sarcomatosis, Sarcoma, Whole abdominopelvic radiotherapy",

author = "Pinnix, {Chelsea C.} and Fontanilla, {Hiral P.} and Andrea Hayes-Jordan and Vivek Subbiah and Bilton, {Stephen D.} and Chang, {Eric L.} and Grosshans, {David R.} and McAleer, {Mary F.} and Sulman, {Eric P.} and Woo, {Shiao Y.} and Peter Anderson and Green, {Holly L.} and Anita Mahajan",

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doi = "10.1016/j.ijrobp.2011.06.1985",

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AU - Pinnix, Chelsea C.

AU - Fontanilla, Hiral P.

AU - Hayes-Jordan, Andrea

AU - Subbiah, Vivek

AU - Bilton, Stephen D.

AU - Chang, Eric L.

AU - Grosshans, David R.

AU - McAleer, Mary F.

AU - Sulman, Eric P.

AU - Woo, Shiao Y.

AU - Anderson, Peter

AU - Green, Holly L.

AU - Mahajan, Anita

PY - 2012/5/1

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N2 - Purpose: Desmoplastic small round cell tumor (DSCRT) is an uncommon pediatric tumor with a poor prognosis. Aggressive multimodality therapy is the current treatment approach; however. treatment toxicity is of concern. We report our results with whole abdominopelvic intensity-modulated radiation therapy (WAP-IMRT) as a component of multimodality therapy for DSCRT at a single institution. Materials/Methods: Medical records of all patients with DSCRT who received WAP-IMRT as part of definitive treatment at MD Anderson (2006-2010) were identified and reviewed. Results: Eight patients with DSRCT received WAP-IMRT with a median follow-up of 15.2 months. All patients received multiple courses of chemotherapy followed by surgical debulking of intra-abdominal disease; seven also had intraoperative hyperthermic cisplatin. WAP-IMRT was delivered to a total dose of 30 Gy postoperatively; four patients received a simultaneous boost (6-10 Gy) to sites of gross residual disease. Seven patients received concurrent chemotherapy during WAP-IMRT. No Radiation Therapy Oncology Group Grade 4 nausea, vomiting, or diarrhea occurred during RT. Red-cell transfusions were given to two patients to maintain hemoglobin levels >10 g/dL. Grade 4 cytopenia requiring growth factor support occurred in only one patient; no other significant cytopenias were noted. WAP-IMRT resulted in 25% lower radiation doses to the lumbosacral vertebral bodies and pelvic bones than conventional RT plans. The median time to local or distant failure after WAP-IMRT was 8.73 months in seven patients. One patient who had completed RT 20 months before the last follow-up remains alive without evidence of disease. Five patients (63%) experienced treatment failure in the abdomen. Distant failure occurred in three patients (37.5%). Conclusions: WAP-IMRT with concurrent radiosensitizing chemotherapy was well tolerated after aggressive surgery for DSCRT. Enhanced bone sparing with IMRT probably accounts for the low hematologic toxicity (vs. conventional WAP-RT). This modality should be considered as an additional local-regional control option for DSRCT.

AB - Purpose: Desmoplastic small round cell tumor (DSCRT) is an uncommon pediatric tumor with a poor prognosis. Aggressive multimodality therapy is the current treatment approach; however. treatment toxicity is of concern. We report our results with whole abdominopelvic intensity-modulated radiation therapy (WAP-IMRT) as a component of multimodality therapy for DSCRT at a single institution. Materials/Methods: Medical records of all patients with DSCRT who received WAP-IMRT as part of definitive treatment at MD Anderson (2006-2010) were identified and reviewed. Results: Eight patients with DSRCT received WAP-IMRT with a median follow-up of 15.2 months. All patients received multiple courses of chemotherapy followed by surgical debulking of intra-abdominal disease; seven also had intraoperative hyperthermic cisplatin. WAP-IMRT was delivered to a total dose of 30 Gy postoperatively; four patients received a simultaneous boost (6-10 Gy) to sites of gross residual disease. Seven patients received concurrent chemotherapy during WAP-IMRT. No Radiation Therapy Oncology Group Grade 4 nausea, vomiting, or diarrhea occurred during RT. Red-cell transfusions were given to two patients to maintain hemoglobin levels >10 g/dL. Grade 4 cytopenia requiring growth factor support occurred in only one patient; no other significant cytopenias were noted. WAP-IMRT resulted in 25% lower radiation doses to the lumbosacral vertebral bodies and pelvic bones than conventional RT plans. The median time to local or distant failure after WAP-IMRT was 8.73 months in seven patients. One patient who had completed RT 20 months before the last follow-up remains alive without evidence of disease. Five patients (63%) experienced treatment failure in the abdomen. Distant failure occurred in three patients (37.5%). Conclusions: WAP-IMRT with concurrent radiosensitizing chemotherapy was well tolerated after aggressive surgery for DSCRT. Enhanced bone sparing with IMRT probably accounts for the low hematologic toxicity (vs. conventional WAP-RT). This modality should be considered as an additional local-regional control option for DSRCT.

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KW - IMRT

KW - Pediatric cancer

KW - Peritoneal sarcomatosis

KW - Sarcoma

KW - Whole abdominopelvic radiotherapy

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Whole abdominopelvic intensity-modulated radiation therapy for desmoplastic small round cell tumor after surgery

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